ERG induces taxane resistance in castration-resistant prostate cancer

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作者
Giuseppe Galletti
Alexandre Matov
Himisha Beltran
Jacqueline Fontugne
Juan Miguel Mosquera
Cynthia Cheung
Theresa Y. MacDonald
Matthew Sung
Sandra O’Toole
James G. Kench
Sung Suk Chae
Dragi Kimovski
Scott T. Tagawa
David M. Nanus
Mark A. Rubin
Lisa G. Horvath
Paraskevi Giannakakou
David S. Rickman
机构
[1] Weill Cornell Medical College,Department of Medicine
[2] University for Information Science and Technology St Paul the Apostle,Department of Pathology and Laboratory Medicine
[3] Institute of Precision Medicine of Weill Cornell Medical College and New York-Presbyterian Hospital,Department of Tissue Pathology and Diagnostic Oncology
[4] Weill Cornell Medical College,Department of Medical Oncology
[5] Royal Prince Alfred Hospital,undefined
[6] Camperdown,undefined
[7] The Kinghorn Cancer Centre / Garvan Institute of Medical Research,undefined
[8] Victoria St,undefined
[9] Darlinghurst,undefined
[10] Weill Cornell Cancer Center,undefined
[11] Chris O’Brien Lifehouse,undefined
[12] Royal Prince Alfred Hospital and the University of Sydney,undefined
[13] Camperdown,undefined
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摘要
Taxanes are the only chemotherapies used to treat patients with metastatic castration-resistant prostate cancer (CRPC). Despite the initial efficacy of taxanes in treating CRPC, all patients ultimately fail due to the development of drug resistance. In this study, we show that ERG overexpression in in vitro and in vivo models of CRPC is associated with decreased sensitivity to taxanes. ERG affects several parameters of microtubule dynamics and inhibits effective drug-target engagement of docetaxel or cabazitaxel with tubulin. Finally, analysis of a cohort of 34 men with metastatic CRPC treated with docetaxel chemotherapy reveals that ERG-overexpressing prostate cancers have twice the chance of docetaxel resistance than ERG-negative cancers. Our data suggest that ERG plays a role beyond regulating gene expression and functions outside the nucleus to cooperate with tubulin towards taxane insensitivity. Determining ERG rearrangement status may aid in patient selection for docetaxel or cabazitaxel therapy and/or influence co-targeting approaches.
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